Plac1 Is a Key Regulator of the Inflammatory Response and Immune Tolerance in Mammary Tumorigenesis

Hongyan Yuan; Xiaoyi Wang; Chunmei Shi; Lu Jin; Jianxia Hu; Alston Zhang; James Li; Nairuthya Vijayendra; Venkata Doodala; Spencer Weiss; Yong Tang; Louis M. Weiner; Robert I. Glazer

doi:10.1038/s41598-018-24022-w

Plac1 Is a Key Regulator of the Inflammatory Response and Immune Tolerance in Mammary Tumorigenesis

Hongyan Yuan, Xiaoyi Wang, Chunmei Shi, Lu Jin, Jianxia Hu, Alston Zhang, James Li, Nairuthya Vijayendra, Venkata Doodala, Spencer Weiss, Yong Tang, Louis M. Weiner, Robert I. Glazer

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16 Scopus citations

Abstract

Plac1 is an X-linked trophoblast gene expressed at high levels in the placenta, but not in adult somatic tissues other than the testis. Plac1 however is re-expressed in several solid tumors and in most human cancer cell lines. To explore the role of Plac1 in cancer progression, Plac1 was reduced by RNA interference in EO771 mammary carcinoma cells. EO771 "knockdown" (KD) resulted in 50% reduction in proliferation in vitro and impaired tumor growth in syngeneic mice; however, tumor growth in SCID mice was equivalent to tumor cells expressing a non-silencing control RNA, suggesting that Plac1 regulated adaptive immunity. Gene expression profiling of Plac1 KD cells indicated reduction in several inflammatory and immune factors, including Cxcl1, Ccl5, Ly6a/Sca-1, Ly6c and Lif. Treatment of mice engrafted with wild-type EO771 cells with a Cxcr2 antagonist impaired tumor growth, reduced myeloid-derived suppressor cells and regulatory T cells, while increasing macrophages, dendritic cells, NK cells and the penetration of CD8+ T cells into the tumor bed. Cxcl1 KD phenocopied the effects of Plac1 KD on tumor growth, and overexpression of Cxcl1 partially rescued Plac1 KD cells. These results reveal that Plac1 modulates a tolerogenic tumor microenvironment in part by modulating the chemokine axis.

Original language	English (US)
Article number	5717
Journal	Scientific reports
Volume	8
Issue number	1
DOIs	https://doi.org/10.1038/s41598-018-24022-w
State	Published - Dec 1 2018
Externally published	Yes

Bibliographical note

Funding Information:
This work was supported by grants from the Nina Hyde Foundation, the Avon Foundation for Women, contract 1NO1 CN43302-WA19 from the National Cancer Institute, NIH, and award 1P30 CA051008 from the National Cancer Institute, NIH, to the Lombardi Comprehensive Cancer Center. This investigation was conducted using the Animal Research, Genomics and Epigenomics, Tissue and Histology and Microscopy and Imaging Shared Resources of the LCCC, and by an animal facilities construction grant from the NIH.

Publisher Copyright:
© 2018 The Author(s).

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title = "Plac1 Is a Key Regulator of the Inflammatory Response and Immune Tolerance in Mammary Tumorigenesis",

abstract = "Plac1 is an X-linked trophoblast gene expressed at high levels in the placenta, but not in adult somatic tissues other than the testis. Plac1 however is re-expressed in several solid tumors and in most human cancer cell lines. To explore the role of Plac1 in cancer progression, Plac1 was reduced by RNA interference in EO771 mammary carcinoma cells. EO771 {"}knockdown{"} (KD) resulted in 50% reduction in proliferation in vitro and impaired tumor growth in syngeneic mice; however, tumor growth in SCID mice was equivalent to tumor cells expressing a non-silencing control RNA, suggesting that Plac1 regulated adaptive immunity. Gene expression profiling of Plac1 KD cells indicated reduction in several inflammatory and immune factors, including Cxcl1, Ccl5, Ly6a/Sca-1, Ly6c and Lif. Treatment of mice engrafted with wild-type EO771 cells with a Cxcr2 antagonist impaired tumor growth, reduced myeloid-derived suppressor cells and regulatory T cells, while increasing macrophages, dendritic cells, NK cells and the penetration of CD8+ T cells into the tumor bed. Cxcl1 KD phenocopied the effects of Plac1 KD on tumor growth, and overexpression of Cxcl1 partially rescued Plac1 KD cells. These results reveal that Plac1 modulates a tolerogenic tumor microenvironment in part by modulating the chemokine axis.",

author = "Hongyan Yuan and Xiaoyi Wang and Chunmei Shi and Lu Jin and Jianxia Hu and Alston Zhang and James Li and Nairuthya Vijayendra and Venkata Doodala and Spencer Weiss and Yong Tang and Weiner, {Louis M.} and Glazer, {Robert I.}",

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AU - Yuan, Hongyan

AU - Wang, Xiaoyi

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AU - Jin, Lu

AU - Hu, Jianxia

AU - Zhang, Alston

AU - Li, James

AU - Vijayendra, Nairuthya

AU - Doodala, Venkata

AU - Weiss, Spencer

AU - Tang, Yong

AU - Weiner, Louis M.

AU - Glazer, Robert I.

N1 - Funding Information: This work was supported by grants from the Nina Hyde Foundation, the Avon Foundation for Women, contract 1NO1 CN43302-WA19 from the National Cancer Institute, NIH, and award 1P30 CA051008 from the National Cancer Institute, NIH, to the Lombardi Comprehensive Cancer Center. This investigation was conducted using the Animal Research, Genomics and Epigenomics, Tissue and Histology and Microscopy and Imaging Shared Resources of the LCCC, and by an animal facilities construction grant from the NIH. Publisher Copyright: © 2018 The Author(s).

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Plac1 Is a Key Regulator of the Inflammatory Response and Immune Tolerance in Mammary Tumorigenesis

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